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交联剂对海藻酸盐基质完整性及药物释放的影响。

Impact of cross-linker on alginate matrix integrity and drug release.

作者信息

Ching A L, Liew C V, Heng P W S, Chan L W

机构信息

Department of Pharmacy, Faculty of Science, National University of Singapore, 18 Science Drive 4, Singapore 117543, Singapore.

出版信息

Int J Pharm. 2008 May 1;355(1-2):259-68. doi: 10.1016/j.ijpharm.2007.12.038. Epub 2008 Jan 5.

Abstract

Sodium alginate, a biopolymer, was employed in the formulation of matrix tablets. They cracked or laminated at acidic pH, compromising their dissolution performance. Improved mechanical strength and reduced barrier permeability of calcium alginate gel provided the rationale for cross-linking the alginate matrix to sustain drug release. Studies had suggested that the incorporation of soluble calcium salts in alginate matrix tablets could sustain drug release at near-neutral pH due to in situ cross-linking. However, results from the present study showed otherwise when gastrointestinal pH conditions were simulated. Significant reduction in drug release rate was only observed when an external calcium source was utilized at low concentration. High calcium ion concentrations caused matrix disintegration. In contrast, matrices pre-coated by calcium alginate could sustain drug release at pH 1.2 followed by pH 6.8 for over 12h. The presence of cross-linked barrier impeded matrix lamination and preserved matrix structure, contributing to at least three-fold reduction in drug release at pH 1.2. Zero order release as well as delayed burst release could be achieved by employing appropriate grade of alginate and cross-linking conditions.

摘要

海藻酸钠,一种生物聚合物,被用于制备骨架片。它们在酸性pH条件下会出现破裂或分层现象,这会影响其溶出性能。海藻酸钙凝胶机械强度的提高和屏障通透性的降低为交联海藻酸盐基质以维持药物释放提供了理论依据。研究表明,在海藻酸盐骨架片中加入可溶性钙盐,由于原位交联作用,可在近中性pH条件下维持药物释放。然而,本研究在模拟胃肠道pH条件时得出了不同的结果。只有在低浓度使用外部钙源时,才观察到药物释放速率显著降低。高钙离子浓度会导致基质崩解。相比之下,用海藻酸钙预包衣的基质在pH 1.2然后pH 6.8的条件下可持续释放药物超过12小时。交联屏障的存在阻碍了基质分层并保持了基质结构,使pH 1.2时的药物释放至少降低了三倍。通过采用适当等级的海藻酸盐和交联条件,可以实现零级释放以及延迟突释。

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